Diagnosis of alcoholic liver disease.
Study Goal
The abstract does not focus on Alanine but rather discusses alcoholic liver disease (ALD) and its diagnosis.
Results Summary
The abstract does not report any findings related to Alanine.
Population
Patients with clinical features of hepatitis, chronic liver disease, or elevated transaminase levels.
Effective Dosage
Not mentioned
Duration
Not mentioned
Interactions
None mentioned
| Intervention | Direction | Endpoint | Population | Dosage | Impact | Claim # |
|---|---|---|---|---|---|---|
Alcohol | increase | spectrum of liver injury | - | - | is associated with | #1 |
Excessive or harmful alcohol use | increase | death and disability | globally | - | is ranked as one of the top five risk factors for | #2 |
Excessive or harmful alcohol use | increase | deaths | - | 2.5 million | results in | #3 |
Excessive or harmful alcohol use | increase | annual disability adjusted life years | - | 69.4 million | results in | #4 |
Alcohol | increase | hepatic steatosis | early ALD | - | characterized by | #5 |
Alcohol | increase | transaminase levels with aspartate aminotransferase greater than alanine aminotransferase | ALD | - | typical laboratory findings include | #6 |
Alcohol | increase | increased mean corpuscular volume | ALD | - | typical laboratory findings include | #7 |
Alcohol | increase | increased gamma-glutamyltranspeptidase | ALD | - | typical laboratory findings include | #8 |
Alcohol | increase | increased IgA to IgG ratio | ALD | - | typical laboratory findings include | #9 |
Alcohol | increase | hepatic steatosis | ALD | - | histological features can ultimately define the diagnosis according to the typical presence and distribution of | #10 |
Alcohol | increase | inflammation | ALD | - | histological features can ultimately define the diagnosis according to the typical presence and distribution of | #11 |
Alcohol | increase | Mallory-Denk bodies | ALD | - | histological features can ultimately define the diagnosis according to the typical presence and distribution of | #12 |
Sobriety | decrease | ALD | - | - | potential reversible nature of ALD with | #13 |
Alcohol is a hepatotoxin that is commonly consumed worldwide and is associated with a spectrum of liver injury including simple steatosis or fatty liver, alcoholic hepatitis, fibrosis, and cirrhosis. Alcoholic liver disease (ALD) is a general term used to refer to this spectrum of alcohol-related liver injuries. Excessive or harmful alcohol use is ranked as one of the top five risk factors for death and disability globally and results in 2.5 million deaths and 69.4 million annual disability adjusted life years. All patients who present with clinical features of hepatitis or chronic liver disease or who have elevated serum elevated transaminase levels should be screened for an alcohol use disorder. The diagnosis of ALD can generally be made based on history, clinical and laboratory findings. However, the diagnosis of ALD can be clinically challenging as there is no single diagnostic test that confirms the diagnosis and patients may not be forthcoming about their degree of alcohol consumption. In addition, clinical findings may be absent or minimal in early ALD characterized by hepatic steatosis. Typical laboratory findings in ALD include transaminase levels with aspartate aminotransferase greater than alanine aminotransferase as well as increased mean corpuscular volume, gamma-glutamyltranspeptidase, and IgA to IgG ratio. In unclear cases, the diagnosis can be supported by imaging and liver biopsy. The histological features of ALD can ultimately define the diagnosis according to the typical presence and distribution of hepatic steatosis, inflammation, and Mallory-Denk bodies. Because of the potential reversible nature of ALD with sobriety, regular screening of the general population and early diagnosis are essential.